Everolimus in the management of metastatic renal cell carcinoma: an evidence-based review of its place in therapy

Core Evidence Pub Date : 2016-09-01 DOI:10.2147/CE.S98687

S. Buti, A. Leonetti, A. Dallatomasina, M. Bersanelli

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引用次数: 42

Abstract

Introduction Renal cell carcinoma (RCC) is the most common type of kidney cancer in adults, and its pathogenesis is strictly related to altered cellular response to hypoxia, in which mTOR signaling pathway is implicated. Everolimus, an mTOR serine/threonine kinase inhibitor, represents a therapeutic option for the treatment of advanced RCC. Aim The objective of this article is to review the evidence for the treatment of metastatic RCC with everolimus. Evidence review Everolimus was approved for second- and third-line therapy in patients with advanced RCC according to the results of a Phase III pivotal trial that demonstrated a benefit in median progression-free survival of ~2 months compared to placebo after failure of previous lines of therapy, of which at least one was an anti-VEGFR tyrosine kinase inhibitor (TKI). The role of this drug in first-line setting has been investigated in Phase II trials, with no significant clinical benefit, even in combination with bevacizumab. Everolimus activity in non-clear cell RCC is supported by two randomized Phase II trials that confirmed the benefit in second-line setting but not in first line. Recently, two randomized Phase III trials (METEOR and CheckMate 025) demonstrated the inferiority of everolimus in second-line setting compared to the TKI cabozantinib and to the immune checkpoint inhibitor nivolumab, respectively. Moreover, a recent Phase II study demonstrated a significant benefit for the second-line combination treatment with everolimus plus lenvatinib (a novel TKI) in terms of progression-free survival and overall survival compared to the single-agent everolimus. Basing on preclinical data, the main downstream effectors of mTOR cascade, S6RP and its phosphorylated form, could be good predictive biomarkers of response to everolimus. The safety profile of the drug is favorable, with a good cost-effectiveness compared to second-line sorafenib or axitinib, and no significant impact on the quality of life of treated patients has been found. Conclusion Everolimus still represents a current standard of treatment for RCC progressive to previous treatment lines with VEGFR-TKI. The evidence about two new molecules, cabozantinib and nivolumab, successfully tested head-to-head with everolimus in recently published Phase III trials, will determine the shift of everolimus to the third-line setting and subsequent lines of treatment.

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依维莫司在转移性肾细胞癌的治疗:其治疗地位的循证回顾

肾细胞癌(RCC)是成人中最常见的肾癌类型，其发病机制与细胞对缺氧反应的改变密切相关，其中涉及mTOR信号通路。依维莫司是一种mTOR丝氨酸/苏氨酸激酶抑制剂，是治疗晚期RCC的一种治疗选择。目的本文的目的是回顾依维莫司治疗转移性肾细胞癌的证据。根据一项III期关键试验的结果，依维莫司被批准用于晚期RCC患者的二线和三线治疗，该试验显示，在先前的治疗失败后，与安慰剂相比，依维莫司的中位无进展生存期为2个月，其中至少有一种是抗vegfr酪氨酸激酶抑制剂(TKI)。该药物在一线环境中的作用已经在II期试验中进行了研究，即使与贝伐单抗联合使用，也没有明显的临床益处。依维莫司在非透明细胞RCC中的活性得到了两项随机II期试验的支持，这两项试验证实了依维莫司在二线治疗中的益处，但在一线治疗中却没有。最近，两项随机III期试验(METEOR和CheckMate 025)分别证明了依维莫司在二线治疗中的劣势，与TKI卡博桑替尼和免疫检查点抑制剂尼武单抗相比。此外，最近的一项II期研究表明，与单药依维莫司相比，依维莫司加lenvatinib(一种新型TKI)的二线联合治疗在无进展生存期和总生存期方面有显著的益处。根据临床前数据，mTOR级联的主要下游效应物S6RP及其磷酸化形式可能是对依维莫司反应的良好预测生物标志物。该药物的安全性良好，与二线索拉非尼或阿西替尼相比具有良好的成本效益，并且未发现对治疗患者的生活质量有显著影响。结论依维莫司仍然是目前的标准治疗进展的RCC与先前的VEGFR-TKI治疗线。在最近发表的III期临床试验中，cabozantinib和nivolumab这两种新分子与依维莫司成功进行了正面测试，这将决定依维莫司向三线治疗和后续治疗的转变。

本文章由计算机程序翻译，如有差异，请以英文原文为准。

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Core Evidence PHARMACOLOGY & PHARMACY-

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期刊介绍： Core Evidence evaluates the evidence underlying the potential place in therapy of drugs throughout their development lifecycle from preclinical to postlaunch. The focus of each review is to evaluate the case for a new drug or class in outcome terms in specific indications and patient groups The emerging evidence on new drugs is reviewed at key stages of development and evaluated against unmet needs